Enhanced antitumor activity of a combination treatment with a mouse/human chimeric anti-MK-1 antibody and lymphokine-activated killer cells in vitro and in a severe combined immunodeficient mouse xenograft model

Yamamoto, Takafumi; Nakamura, Ken; Senba, Tarumi; Tomita, Yoshihiro; Ikeda, Seiyo; Kuroki, Masahide

doi:10.1007/s002620050561

Cited by 8 publications

(5 citation statements)

References 31 publications

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“…In addition, a mouse/human chimeric anti-MK-1 antibody in combination with IL-2 was injected intravenously. Sixteen days later the animals were sacrificed and a reduction in subcutaneous tumor mass of approximately 70% was found compared to the untreated controls [22]. In keeping with these findings, tumor mass reduction after immunotherapy with 17-1A mAb could also be realized in the presented model.…”

Section: Discussionsupporting

confidence: 58%

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Prevention of Peritoneal Carcinomatosis from Human Gastric Cancer Cells by Adjuvant-Type Intraperitoneal Immunotherapy in a SCID Mouse Model

Piso¹,

Aselmann²,

Wasielewski

et al. 2003

Eur Surg Res

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Purpose: We analyzed the effect of intraperitoneal immunotherapy in an animal model mimicking locoregional dissemination of tumor cells during resection of advanced tumors. Methods: We first established a tumor model with human gastric cancer cells (MKN-45) in the peritoneal cavity of CB-17-SCID mice. Three hours following the injection of tumor cells into the peritoneal cavity, mAb 17-1A alone and in combination with human LAK cells were given intraperitoneally at different dosages. The results were quantified by determining the weight of the peritoneal tumor masses. Results: After intraperitoneal administration of 17-1A mAb, a tumor reduction could be shown (median tumor mass after 10 µg mAb: 171 µg; after 100 µg: 130 µg) when compared with the control group (632 µg). Following a combined therapy with mAb and LAK cells, a statistically significant tumor reduction could be observed (after 10 µg mAb + 20–50 × 10⁶ LAK cells: 80 µg; after 100 µg mAb + 20–50 × 10⁶ LAK cells: 12 µg, p = 0.0005). With specific dosages of antibody and LAK cells it was even possible to achieve complete tumor clearance. Conclusions: Intraperitoneal immunotherapy reduces the peritoneal tumor masses and can even prevent the peritoneal carcinomatosis formation.

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Section: Discussionsupporting

confidence: 58%

“…From cell lines of gastric cancer used so far, we chose the line MKN-45 as this cell line expresses 17-1A antigen, and has also been established for the induction of peritoneal carcinomatosis [2, 17, 22]. The antigen 17-1A is a membrane-glycoprotein and belongs to the family of epithelial cellular adhesion molecules (Ep-CAM).…”

Section: Introductionmentioning

confidence: 99%

Prevention of Peritoneal Carcinomatosis from Human Gastric Cancer Cells by Adjuvant-Type Intraperitoneal Immunotherapy in a SCID Mouse Model

Piso¹,

Aselmann²,

Wasielewski

et al. 2003

Eur Surg Res

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“…In some cases, chimeric mouse-human antibodies (129)(130)(131)(132), consisting of murine variable (V)regions and human constant (C)-regions, are employed since "humanized" antibodies are thought to be preferable for treating cancer patients clinically. The mechanism responsible for the anti-tumor effect observed in these systems is antibody-dependent cellular cytotoxicity (ADCC), mediated either by resident host cells (e.g.…”

Section: Antibody-based Therapies Tested In Scid-hu Models Of Cancer mentioning

confidence: 99%

“…The mechanism responsible for the anti-tumor effect observed in these systems is antibody-dependent cellular cytotoxicity (ADCC), mediated either by resident host cells (e.g. NK, macrophage, eosinophils) (126-128, 130, 131), or by adoptively-transferred human effector cells (PBL,LAK) (129,132) or a combination of both. Of specific note is the use of anti-human CD40 antibodies for the treatment of human B-cell lymphoma xenografts, since ligation of CD40 on lymphoma cells has direct anti-proliferative effects in addition to mediating ADCC (126, 133).…”

Section: Antibody-based Therapies Tested In Scid-hu Models Of Cancer mentioning

confidence: 99%

SCID mouse models to study human cancer pathogenesis and approaches to therapy: potential, limitations, and future directions

Richard¹

2002

Front Biosci

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The successful engraftment of human tumors and human immunocompetent cells into severe combined immunodeficient (SCID) mice has led to the generation of a wide array of different experimental designs that have proven useful in studying the cell biology of human cancer, and for evaluating novel therapeutic approaches to the treatment of cancer. In this review five of the most frequently used embodiments of the SCID model are presented. The goals of this review are to discuss how each model has been utilized to study human cancer and its response to many different novel therapies, to provide an assessment of the strengths and limitations of each model, and to outline future directions with a focus on what is needed to overcome some of the current limitations and pitfalls of the SCID models.

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“…2) In combination with human lymphokine-activated killer cells, Ch FU-MK-1 showed a marked growth inhibition of human MK-1-producing tumor cells in vitro and in severe combined immunodeficiency mice. 3) The histochemical distribution of the MK-1 antigen is similar to the known distributions of a number of carcinoma-associated antigens, such as the 17-1A antigen defined by MAb CO17-1A, 4,5) the Trop-1 antigen 6,7) iden-tified by MAb 162-21.2, the KS1/4 antigen or KSA recognized by MAb KS1/4, [8][9][10] the GA733-2 antigen specified by MAb GA733, 11,12) epithelial glycoprotein-2 (EGP-2) defined by MAb HEA125, 13,14) and the C215 antigen identified by MAb C215. 15,16) These antigens are expressed to varying degrees in epithelial carcinomas such as gastric, colonic, pancreatic, and mammary cancers.…”

mentioning

confidence: 99%

Molecular Identification of a Human Carcinoma‐associated Glycoprotein Antigen Recognized by Mouse Monoclonal Antibody FU‐MK‐1

Tomita

Yamamoto

Kuwahara

et al. 2000

Japanese Journal of Cancer Research

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Enhanced antitumor activity of a combination treatment with a mouse/human chimeric anti-MK-1 antibody and lymphokine-activated killer cells in vitro and in a severe combined immunodeficient mouse xenograft model

Cited by 8 publications

References 31 publications

Prevention of Peritoneal Carcinomatosis from Human Gastric Cancer Cells by Adjuvant-Type Intraperitoneal Immunotherapy in a SCID Mouse Model

Prevention of Peritoneal Carcinomatosis from Human Gastric Cancer Cells by Adjuvant-Type Intraperitoneal Immunotherapy in a SCID Mouse Model

SCID mouse models to study human cancer pathogenesis and approaches to therapy: potential, limitations, and future directions

Molecular Identification of a Human Carcinoma‐associated Glycoprotein Antigen Recognized by Mouse Monoclonal Antibody FU‐MK‐1

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